Design, Synthesis, and Pharmacological Evaluation of Second-Generation Tetrahydroisoquinoline-Based CXCR4 Antagonists with Favorable ADME Properties

Nguyen, Huy H.; Kim, Michelle B.; Wilson, Robert J.; Butch, Christopher J.; Kuo, Katie M.; Miller, Eric J; Tahirovic, Yesim A.; Jecs, Edgars; Truax, Valarie M.; Wang, Tao; Sum, Chi Shing; Cvijic, Mary Ellen; Schroeder, G.; Wilson, Lawrence J.; Liotta, Dennis

doi:10.1021/acs.jmedchem.8b00450

Cited by 21 publications

(15 citation statements)

References 76 publications

Supporting

Mentioning

Contrasting

Order By: Relevance

“…Tetrahydroisoquinoline and isoindoline are nitrogen‐fused heterocyclic ring structures that exist in many bioactive molecules including natural products and commercially available pharmaceuticals 21 . Thus, the discovery of a novel synthetic method for tetrahydroisoquinoline and isoindoline is valuable for drug discovery, thus this reaction protocol using TiCl 4 and TBD was applied for preparation of nitrogen‐fused heterocyclic ring structures (Table 4).…”

Section: Resultsmentioning

confidence: 99%

Facile titanium(IV) chloride and TBD‐mediated synthesis of N‐aryl‐substituted azacycles from arylhydrazines

Tran

Hong

Kim

2022

Bulletin Korean Chem Soc

View full text Add to dashboard Cite

A novel practical synthesis of N-aryl-substituted azacycles from arylhydrazines is described. In this method, target azacycles were prepared via reaction of arylhydrazines with cyclic ethers in the presence of both titanium(IV) chloride and 1,5,7-triazabicyclo[4.4.0]dec-5-ene (TBD) as key combined reagents. Using this synthetic protocol with titanium(IV) chloride and TBD, reaction of arylhydrazines with cyclic ethers successfully afforded various N-aryl-substituted azacycles in high yield. This facile synthetic method using arylhydrazines will be a promising guide for the synthesis of azacycles from arylhydrazines.

show abstract

Section: Resultsmentioning

confidence: 99%

Facile titanium(IV) chloride and TBD‐mediated synthesis of N‐aryl‐substituted azacycles from arylhydrazines

Tran

Hong

Kim

2022

Bulletin Korean Chem Soc

View full text Add to dashboard Cite

show abstract

“…Substitution of the bicyclic heteroaromatic moiety by a partially saturated ring system yielded the tetrahydroisoquinoline derivative 5 (also known as TIQ15, Figure 1 ), which is a highly potent and selective CXCR4 antagonist [ 15 ]. Further optimization yielded compound 6 , which has improved in vitro ADME properties compared to compound 5 [ 16 ]. In contrast to the lower part, the upper tetrahydroquinoline moiety of AMD-11070 has been left relatively unexplored.…”

Section: Introductionmentioning

confidence: 99%

Synthesis and Anti-HIV Activity of a Novel Series of Isoquinoline-Based CXCR4 Antagonists

et al. 2021

View full text Add to dashboard Cite

An expansion of the structure–activity relationship study of CXCR4 antagonists led to the synthesis of a series of isoquinolines, bearing a tetrahydroquinoline or a 3-methylpyridinyl moiety as head group. All compounds were investigated for CXCR4 affinity and antagonism in competition binding and calcium mobilization assays, respectively. In addition, the anti-HIV activity of all analogues was determined. All compounds showed excellent activity, with compound 24c being the most promising one, since it displayed consistently low nanomolar activity in the various assays.

show abstract

“…CXCR4 is one of 23 known human chemokine receptors, which plays a key role in leukocyte trafficking, hematopoiesis, organ development and cancer metastases (Zweemer et al, 2014). It was revealed that CXCR4 is associated with more than 23 types of cancers (Wu et al, 2010; Nguyen et al, 2018). CXCR4 and related CC chemokine receptor 5 (CCR5) are not only the key regulators of signal transduction, but also involve in the entry of HIV-1 virus as coreceptors of HIV-1 into leukocytes (Shaik et al, 2019).…”

Section: Introductionmentioning

confidence: 99%

Probing the Druggablility on the Interface of the Protein–Protein Interaction and Its Allosteric Regulation Mechanism on the Drug Screening for the CXCR4 Homodimer

et al. 2019

View full text Add to dashboard Cite

Modulating protein–protein interactions (PPIs) with small drug-like molecules targeting it exhibits great promise in modern drug discovery. G protein-coupled receptors (GPCRs) are the largest family of targeted proteins and could form dimers in living biological cells through PPIs. However, compared to drug development of the orthosteric site, there has been lack of investigations on the druggability of the PPI interface for GPCRs and its functional implication on experiments. Thus, in order to address these issues, we constructed a novel computational strategy, which involved in molecular dynamics simulation, virtual screening and protein structure network (PSN), to study one representative GPCR homodimer (CXCR4). One druggable pocket was identified in the PPI interface and one small molecule targeting it was screened, which could strengthen PPI mainly through hydrophobic interaction between the benzene rings of the PPI molecule and TM4 of the receptor. The PSN results further reveals that the PPI molecule could increase the number of the allosteric regulation pathways between the druggable pocket of the dimer interface to the orthostatic site for the subunit A but only play minor role for the other subunit B, leading to the asymmetric change in the volume of the binding pockets for the two subunits (increase for the subunit A and minor change for the subunit B). Consequently, the screening performance of the subunit A to the antagonists is enhanced while the subunit B is unchanged nearly, implying that the PPI molecule may be beneficial to enhance the drug efficacies of the antagonists. In addition, one main regulation pathway with the highest frequency was identified for the subunit A, which consists of Trp1955.34–Tyr190ECL2–Val1965.35–Gln2005.39–Asp2626.58–Cys28N-term, revealing their importance in the allosteric regulation from the PPI molecule. The observations from the work could provide valuable information for the development of the PPI drug-like molecule for GPCRs.

show abstract

Design, Synthesis, and Pharmacological Evaluation of Second-Generation Tetrahydroisoquinoline-Based CXCR4 Antagonists with Favorable ADME Properties

Cited by 21 publications

References 76 publications

Facile titanium(IV) chloride and TBD‐mediated synthesis of N‐aryl‐substituted azacycles from arylhydrazines

Facile titanium(IV) chloride and TBD‐mediated synthesis of N‐aryl‐substituted azacycles from arylhydrazines

Synthesis and Anti-HIV Activity of a Novel Series of Isoquinoline-Based CXCR4 Antagonists

Probing the Druggablility on the Interface of the Protein–Protein Interaction and Its Allosteric Regulation Mechanism on the Drug Screening for the CXCR4 Homodimer

Contact Info

Product

Resources

About